E control mice were infected by subcutaneous injection of 750 L3 N. brasiliensis larvae. Parasite egg CUDC-907 site production was determined on days 6?4 PI (Figure 1 A) and intestinal adult worm burdens determined on days 7 and 10 PI (Figure 1B and FigureIL-4Ra-Mediated Intestinal HypercontractilityS1). Heterozygous IL-4Ra2/lox control and iLckcreIL-4Ra2/lox mice showed similar egg production throughout the infection with egg counts peaking at day 7 and clearing by day 9 post infection (PI). Intestinal worm burdens in both mice strains were similar at day 7 PI and absent by day 10 PI. As previously demonstrated, IL4Ra2/2 mice did not clear infection efficiently showing a maintained egg production at day 11 PI and the presence of adult worms detected at day 10 PI [20,24]. As seen in previously described CD4+ T cell-specific IL-4Ra deficient mice (LckcreIL4Ra2/lox) [28], pan T cell-specific IL-4Ra deficient mice efficiently clear the worms similar to IL-4Ra-responsive control mice. T cell subpopulations other than CD4+ T cells are also known to play a key role in N. brasiliensis clearance, such as cd T cells which initiate rapid expulsion of adult worms from the intestine and limit egg production [35]. To determine if IL-4Ra surface expression on CD8+, cd and NK T cells plays a role in N. brasiliensis expulsion we compared pan T cell-specific IL-4Ra deficient mice (iLckcreIL-4Ra2/lox) described in this paper with the previously described CD4+ T cell-specific IL-4Ra deficient (LckcreIL-4Ra2/lox) mice which have partial or normal IL-4Ra surface expression on CD8+, cd and NK T cells (Table S1). Both strains showed comparable worm expulsion, egg numbers and IL13 production (Figure S2 A ) therefore we concluded that IL4Ra-responsive T cells are not crucial for N. brasiliensis expulsion. Furthermore, to determine the influence of loxP insertion on IL4 receptor function we compared N. brasiliensis infected WT BALB/c mice with heterozygous IL-4Ra2/lox control mice and found no difference (Figure S3 A ). These results suggest that neither loss of one IL-4Ra allele nor silent mutation due to lox insertion has a significant effect on acetylcholine-mediated contraction.of the TH2 cytokines, IL-4 and IL-13, reduced TH1 associated IFN-c and TH17 associated IL-17 when compared to the IL-4Raunresponsive CD4+ T cells from IL-4Ra2/2 mice (20,24) (Figure 3A). Interestingly, CD4+ T cells derived from iLckcreIL4Ra2/lox mice showed a similar reduction of IL-4 as CD4+ T cells derived from IL-4Ra2/2 mice). However, IL-13 and IL-17 secretion by iLckcreIL-4Ra2/lox mice was not significantly different to control mice (Figure 3A). Together, these data suggest that IL-4 but not IL-13 responses require IL-4-promoted TH2 cells during N. brasiliensis infection in CD4+ T cells from R7227 mesenteric lymph nodes. To determine levels of IL-4 and IL-13 in the jejunum, soluble homogenates of tissue were analysed by ELISA. As expected, N. brasiliensis infection induced the TH2 cytokines IL-4 and IL-13 in the jejunum of IL-4Ra2/lox control mice (Figure 3B). In contrast, T cell-specific IL-4Ra deficient mice showed impaired IL-4 and IL-13 cytokine response of equivalent magnitude to IL-4Ra2/2 mice. These results are supported by our previous study where mediastinal lymph node CD4+ T cells from mice lacking IL-4Ra expression specifically on CD4+ T cells (LckcreIL-4Ra2/lox) maintained their ability to produce 12926553 IL-13 in contrast to the CD4+ T cells isolated from digested lung [28]. Together these resu.E control mice were infected by subcutaneous injection of 750 L3 N. brasiliensis larvae. Parasite egg production was determined on days 6?4 PI (Figure 1 A) and intestinal adult worm burdens determined on days 7 and 10 PI (Figure 1B and FigureIL-4Ra-Mediated Intestinal HypercontractilityS1). Heterozygous IL-4Ra2/lox control and iLckcreIL-4Ra2/lox mice showed similar egg production throughout the infection with egg counts peaking at day 7 and clearing by day 9 post infection (PI). Intestinal worm burdens in both mice strains were similar at day 7 PI and absent by day 10 PI. As previously demonstrated, IL4Ra2/2 mice did not clear infection efficiently showing a maintained egg production at day 11 PI and the presence of adult worms detected at day 10 PI [20,24]. As seen in previously described CD4+ T cell-specific IL-4Ra deficient mice (LckcreIL4Ra2/lox) [28], pan T cell-specific IL-4Ra deficient mice efficiently clear the worms similar to IL-4Ra-responsive control mice. T cell subpopulations other than CD4+ T cells are also known to play a key role in N. brasiliensis clearance, such as cd T cells which initiate rapid expulsion of adult worms from the intestine and limit egg production [35]. To determine if IL-4Ra surface expression on CD8+, cd and NK T cells plays a role in N. brasiliensis expulsion we compared pan T cell-specific IL-4Ra deficient mice (iLckcreIL-4Ra2/lox) described in this paper with the previously described CD4+ T cell-specific IL-4Ra deficient (LckcreIL-4Ra2/lox) mice which have partial or normal IL-4Ra surface expression on CD8+, cd and NK T cells (Table S1). Both strains showed comparable worm expulsion, egg numbers and IL13 production (Figure S2 A ) therefore we concluded that IL4Ra-responsive T cells are not crucial for N. brasiliensis expulsion. Furthermore, to determine the influence of loxP insertion on IL4 receptor function we compared N. brasiliensis infected WT BALB/c mice with heterozygous IL-4Ra2/lox control mice and found no difference (Figure S3 A ). These results suggest that neither loss of one IL-4Ra allele nor silent mutation due to lox insertion has a significant effect on acetylcholine-mediated contraction.of the TH2 cytokines, IL-4 and IL-13, reduced TH1 associated IFN-c and TH17 associated IL-17 when compared to the IL-4Raunresponsive CD4+ T cells from IL-4Ra2/2 mice (20,24) (Figure 3A). Interestingly, CD4+ T cells derived from iLckcreIL4Ra2/lox mice showed a similar reduction of IL-4 as CD4+ T cells derived from IL-4Ra2/2 mice). However, IL-13 and IL-17 secretion by iLckcreIL-4Ra2/lox mice was not significantly different to control mice (Figure 3A). Together, these data suggest that IL-4 but not IL-13 responses require IL-4-promoted TH2 cells during N. brasiliensis infection in CD4+ T cells from mesenteric lymph nodes. To determine levels of IL-4 and IL-13 in the jejunum, soluble homogenates of tissue were analysed by ELISA. As expected, N. brasiliensis infection induced the TH2 cytokines IL-4 and IL-13 in the jejunum of IL-4Ra2/lox control mice (Figure 3B). In contrast, T cell-specific IL-4Ra deficient mice showed impaired IL-4 and IL-13 cytokine response of equivalent magnitude to IL-4Ra2/2 mice. These results are supported by our previous study where mediastinal lymph node CD4+ T cells from mice lacking IL-4Ra expression specifically on CD4+ T cells (LckcreIL-4Ra2/lox) maintained their ability to produce 12926553 IL-13 in contrast to the CD4+ T cells isolated from digested lung [28]. Together these resu.
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